Absolute Quantitative Targeted Monitoring of Potential Plasma Protein Biomarkers: A Pilot Study on Healthy Individuals.

IF 3.9 3区 工程技术 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY Biomedicines Pub Date : 2024-10-21 DOI:10.3390/biomedicines12102403
Alexey S Kononikhin, Natalia L Starodubtseva, Alexander G Brzhozovskiy, Alisa O Tokareva, Daria N Kashirina, Natalia V Zakharova, Anna E Bugrova, Maria I Indeykina, Liudmila Kh Pastushkova, Irina M Larina, Vladimir A Mitkevich, Alexander A Makarov, Evgeny N Nikolaev
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Abstract

Background/objectives: The development of blood tests for the early detection of individual predisposition to socially significant diseases remains a pressing issue.

Methods: In this pilot study, multiple reaction monitoring mass spectrometry (MRM-MS) with a BAK-270 assay was applied for protein concentrations analysis in blood plasma from 21 healthy volunteers of the European cohort.

Results: The levels of 138 plasma proteins were reliably and precisely quantified in no less than 50% of samples. The quantified proteins included 66 FDA-approved markers of cardiovascular diseases (CVD), and other potential biomarkers of pathologies such as cancer, diabetes mellitus, and Alzheimer's disease. The analysis of individual variations of the plasma proteins revealed significant differences between the male (11) and female (10) groups. In total, fifteen proteins had a significantly different concentration in plasma; this included four proteins that exhibited changes greater than ±1.5-fold, three proteins (RBP4, APCS, and TTR) with higher levels in males, and one (SHBG) elevated in females. The obtained results demonstrated considerable agreement with the data collected from 20 samples of a North American cohort, which were analyzed with the similar MRM assay. The most significant differences between the cohorts of the two continents were observed in the level of 42 plasma proteins (including 24 FDA markers), of which 17 proteins showed a ≥1.5-fold change, and included proteins increased in North Americans (APOB, CRTAC1, C1QB, C1QC, C9, CRP, HP, IGHG1, IGKV4-1, SERPING1, RBP4, and AZGP1), as well as those elevated in Europeans (APOF, CD5L, HBG2, SELPLG, and TNA).

Conclusions: The results suggest a different contribution of specific (patho)physiological pathways (e.g., immune system and blood coagulation) to the development of socially significant diseases in Europeans and North Americans, and they should be taken into account when refining diagnostic panels.

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潜在血浆蛋白生物标记物的绝对定量定向监测:对健康人的试点研究
背景/目标:开发用于早期检测个人易患社会重大疾病的血液检测方法仍然是一个紧迫的问题:在这项试验性研究中,采用 BAK-270 分析法的多反应监测质谱法(MRM-MS)分析了欧洲队列中 21 名健康志愿者血浆中的蛋白质浓度:结果:在不少于 50%的样本中,138 种血浆蛋白质的含量得到了可靠而精确的定量。被量化的蛋白质包括 66 种美国食品及药物管理局批准的心血管疾病(CVD)标志物,以及癌症、糖尿病和阿尔茨海默病等病症的其他潜在生物标志物。对血浆蛋白质个体差异的分析表明,男性组(11 种)和女性组(10 种)之间存在显著差异。共有 15 种蛋白质在血浆中的浓度存在明显差异,其中 4 种蛋白质的变化超过 ±1.5倍,3 种蛋白质(RBP4、APCS 和 TTR)在男性中的含量较高,1 种蛋白质(SHBG)在女性中的含量升高。所获得的结果与从北美队列的 20 份样本中收集的数据相当吻合,后者是通过类似的 MRM 分析法进行分析的。两大洲队列中 42 种血浆蛋白质(包括 24 种 FDA 标志物)的水平差异最大,其中 17 种蛋白质的变化≥1.5倍的变化,其中包括北美人增加的蛋白质(APOB、CRTAC1、C1QB、C1QC、C9、CRP、HP、IGHG1、IGKV4-1、SERPING1、RBP4和AZGP1)以及欧洲人升高的蛋白质(APOF、CD5L、HBG2、SELPLG和TNA):这些结果表明,欧洲人和北美人的特定(病理)生理途径(如免疫系统和血液凝固)对社会重大疾病的发生有不同的作用,在完善诊断面板时应考虑到这些因素。
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来源期刊
Biomedicines
Biomedicines Biochemistry, Genetics and Molecular Biology-General Biochemistry,Genetics and Molecular Biology
CiteScore
5.20
自引率
8.50%
发文量
2823
审稿时长
8 weeks
期刊介绍: Biomedicines (ISSN 2227-9059; CODEN: BIOMID) is an international, scientific, open access journal on biomedicines published quarterly online by MDPI.
期刊最新文献
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